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A Dynamic Spatiotemporal Extracellular Matrix Facilitates Epicardial-Mediated Vertebrate Heart Regeneration

机译:动态时空细胞外基质促进心外膜介导的脊椎动物心脏再生。

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摘要

Unlike humans, certain adult vertebrates such as newts and zebrafish possess extraordinary abilities to functionally regenerate lost appendages and injured organs, including cardiac muscle. Here, we present new evidence that a remodeled extracellular matrix (ECM) directs cell activities essential for cardiac muscle regeneration. Comprehensive mining of DNA microarrays and Gene Ontology term enrichment analyses for regenerating newt and zebrafish hearts revealed that distinct ECM components and ECM-modifying proteases are among the most significantly enriched genes in response to local injury. In contrast, data analyses for mammalian cardiac injury models indicated that inflammation and metabolic processes are the most significantly activated gene groups. In the regenerating newt heart, we show dynamic spatial and temporal changes in tenascin-C, hyaluronic acid, and fibronectin ECM distribution as early as 3 days postamputation. Linked to distinct matrix remodeling, we demonstrate a myocardium-wide proliferative response and radial migration of progenitor cells. In particular, we report dramatic upregulation of a regeneration-specific matrix in the epicardium that precedes the accumulation and migration of progenitor cells. For the first time, we show that the regenerative ECM component tenascin-C significantly increases newt cardiomyocyte cell cycle reentry in vitro. Thus, the engineering of nature-tested extracellular matrices may provide new strategic opportunities for the enhancement of regenerative responses in mammals.
机译:与人类不同,某些成年脊椎动物,例如new和斑马鱼具有非凡的功能,可以在功能上再生丢失的肢体和受伤的器官,包括心肌。在这里,我们提出了新的证据,即重构的细胞外基质(ECM)指导着心肌再生所必需的细胞活动。 DNA微阵列的全面挖掘和用于再生new和斑马鱼心脏的Gene Ontology术语富集分析表明,不同的ECM成分和ECM修饰蛋白酶是响应局部损伤的最显着富集的基因之一。相反,对哺乳动物心脏损伤模型的数据分析表明,炎症和代谢过程是最显着激活的基因组。在再生的t心脏中,我们在截肢后3天就显示出腱生蛋白C,透明质酸和纤连蛋白ECM分布的动态时空变化。链接到不同的基质重塑,我们证明了心肌细胞的增殖反应和祖细胞的径向迁移。特别地,我们报道了在祖细胞的积累和迁移之前,心外膜中再生特异性基质的急剧上调。首次,我们显示了再生ECM成分腱生蛋白C在体外显着增加了newt心肌细胞周期的折返。因此,经过自然测试的细胞外基质的工程化可能为增强哺乳动物的再生反应提供新的战略机会。

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